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Naturally Occurring Molecule Rivals Ozempic in Weight Loss - News Directory 3

Naturally Occurring Molecule Rivals Ozempic in Weight Loss

March 6, 2025 Catherine Williams Health
News Context
At a glance
  • Researchers have identified a ⁤novel ⁣peptide,named BRP,that demonstrates notable potential in reducing ⁤food intake adn promoting fat loss.
  • The discovery⁣ process relied heavily⁣ on advanced computational tools.
  • While the GLP-1 peptide increased neuronal cell activity threefold, a small peptide consisting of just 12 amino acids boosted the cells’ activity tenfold.
Original source: med.stanford.edu

Novel Peptide BRP Shows ⁤Promise in Obesity Treatment

Table of Contents

  • Novel Peptide BRP Shows ⁤Promise in Obesity Treatment
    • Discovery of BRP: A New Hope for obesity Management
    • BRP Outperforms GLP-1‍ in Activating Neuronal Cells
    • impact of BRP on Animal Models
    • No Adverse Behavioral Changes Observed
    • Future Research ⁢Directions
      • The Urgent Need for Effective Obesity Treatments
    • Collaborative⁢ Effort⁢ and Funding
  • BRP: A Novel‍ Peptide Therapy for Obesity – Your Questions Answered
    • What is BRP and⁣ how was it discovered?
    • How does BRP compare to GLP-1 and Semaglutide?
    • What are the effects of BRP on animal models?
    • Are⁢ there any observed side effects of BRP in animal‍ models?
    • How does BRP work? What are its action pathways?
    • What is the potential of BRP as an anti-obesity treatment?
    • What are the next steps in BRP research?
    • Who is ⁢involved in the BRP research?
    • What funding sources support this research?
    • Are there any conflicts of interest to be ‍aware of?

Researchers have identified a ⁤novel ⁣peptide,named BRP,that demonstrates notable potential in reducing ⁤food intake adn promoting fat loss. This revelation could pave the way for new and more⁢ effective anti-obesity medications.

Discovery of BRP: A New Hope for obesity Management

The discovery⁣ process relied heavily⁣ on advanced computational tools. according to Svensson, “The algorithm was absolutely key to our findings.” The Peptide Predictor tool predicted that prohormone⁣ convertase⁤ 1/3 would generate 2,683 unique⁣ peptides from 373 proteins. The focus then shifted to⁢ identifying sequences‍ with biological⁤ activity in the brain. Researchers Coassolo and Svensson screened ‍100 peptides, including GLP-1, for their ability to activate lab-grown neuronal cells.


Peptide Structure

Molecular structure of BRP peptide.

BRP Outperforms GLP-1‍ in Activating Neuronal Cells

While the GLP-1 peptide increased neuronal cell activity threefold, a small peptide consisting of just 12 amino acids boosted the cells’ activity tenfold. This new peptide was named BRP, derived from its⁣ parent prohormone, BPM/retinoic acid inducible neural specific 2, or BRINP2 (BRINP2-related-peptide).

impact of BRP on Animal Models

The effects of BRP were tested⁣ on lean⁤ mice and minipigs, the latter chosen for their metabolic similarities to humans. An intramuscular injection of BRP prior ⁢to feeding reduced ⁢food intake by up to 50% in both animal models over the next⁣ hour. Furthermore,obese mice treated with⁣ daily injections of BRP for ⁣14 days experienced an average weight loss of 3 grams,primarily due ⁢to fat loss,while control animals gained about 3 grams. These mice also showed improved glucose and insulin tolerance.

Animal Model Treatment result
Lean Mice & Minipigs Intramuscular BRP Injection Up to 50% reduction in food intake
Obese Mice Daily BRP Injections (14 days) Average loss of 3 grams (fat loss)
Summary of BRP treatment effects on animal ⁣models.

No Adverse Behavioral Changes Observed

Behavioral studies on the mice ⁣and pigs ‍revealed no significant differences in movements, water intake, anxiety-like behavior, or fecal production. Additional studies of physiological⁤ and brain activity indicated that BRP activates metabolic and neuronal pathways distinct ⁢from those activated by GLP-1 or semaglutide.

Future Research ⁢Directions

Researchers are ⁢now focused on identifying the cell-surface receptors that⁤ bind BRP and further dissecting its action pathways. They are also⁣ exploring methods to prolong the peptide’s effects, aiming for a more convenient dosing schedule if BRP proves effective in regulating human body weight.

The Urgent Need for Effective Obesity Treatments

The search for effective obesity treatments remains a critical area of research. As Svensson notes, “The lack of ⁣effective drugs to treat obesity in humans has been a problem for decades. Nothing we’ve tested before has compared to semaglutide’s ability to decrease appetite and body weight. We are very eager to learn if it is ‍indeed safe and⁣ effective in humans.”

Collaborative⁢ Effort⁢ and Funding

Researchers⁢ from the University ⁢of⁣ California, ‍Berkeley; the‍ University ⁣of Minnesota; and the University of British Columbia contributed to the work.

The study received funding from various sources, including the National ‍Institutes of Health⁤ (grants R01DK125260, P30DK116074, K99AR081618 and GM113854), the SPARK Translational Research Program at Stanford, ⁢Stanford Bio-X, the Stanford ‍Maternal and Child Health Research Institute, the‍ American Heart Association,⁢ a Stanford Medicine⁤ Dean’s Fellowship Award, the Carlsberg Foundation, and the Wu Tsai Human Performance Alliance.

Disclaimer: Svensson and Coassolo are inventors on patents regarding BRP peptides for metabolic disorders. Svensson is a co-founder of Merrifield Therapeutics.


BRP: A Novel‍ Peptide Therapy for Obesity – Your Questions Answered

This article explores the exciting potential of BRP, a novel peptide showing ⁣promise in obesity treatment. We’ll answer your questions and discuss its revelation, effects,‍ and future.

What is BRP and⁣ how was it discovered?

BRP stands for BRINP2-related peptide. It’s a novel 12-amino acid peptide derived from the⁢ prohormone BPM/retinoic acid inducible neural specific⁣ 2 (BRINP2).

Discovery:

Researchers used a “Peptide Predictor” tool to analyze 373 proteins and predict 2,683 unique peptides generated by prohormone convertase 1/3.

They focused on identifying sequences with biological activity in the⁢ brain.

⁤ Coassolo and Svensson screened ⁣100 peptides, including GLP-1,‍ for their ability to activate lab-grown‍ neuronal cells.

BRP outperformed GLP-1,increasing neuronal cell⁣ activity tenfold compared to GLP-1’s threefold‍ increase. This significant ‍difference pointed to BRP’s potential.

How does BRP compare to GLP-1 and Semaglutide?

While both BRP and GLP-1 activate neuronal cells, BRP shows a ‍significantly stronger response ⁣in initial lab tests (tenfold increase in activation vs. threefold ⁢for GLP-1). Moreover, studies suggest‍ BRP activates metabolic and⁢ neuronal ‍pathways distinct from those activated by GLP-1 or semaglutide.

What are the effects of BRP on animal models?

BRP has shown⁢ promising results in animal studies:

Reduced Food Intake: Intramuscular injections of BRP in lean mice ⁢and ‍minipigs reduced food intake by up ⁢to 50% within an hour.

Weight Loss: obese ⁣mice treated with daily BRP injections for 14 days⁣ experienced an average weight loss of 3 grams, primarily from fat loss. Control animals gained‍ weight.

Improved Glucose ⁢and Insulin Tolerance: Obese mice treated with BRP also showed improvements in glucose and insulin tolerance.

| Animal Model⁤ ⁢ | Treatment ⁣ ⁤ | Result ‍ ⁣ ‍ ⁢ ‍ ⁤ ⁢ |

|⁢ :——————- |⁣ :—————————– |⁤ :—————————————— |

| Lean Mice & Minipigs | Intramuscular BRP Injection |⁢ Up to 50% reduction in food intake ‍ |

| Obese‍ Mice ⁢ | Daily⁣ BRP Injections (14‍ days) | Average loss of 3 grams (primarily fat loss) |

Are⁢ there any observed side effects of BRP in animal‍ models?

So far, behavioral studies in mice and pigs have not revealed any significant adverse effects:

No differences in movements, ⁤water intake, or anxiety-like behavior were observed.

Fecal⁢ production remained normal.

How does BRP work? What are its action pathways?

Researchers are still working to fully understand BRP’s mechanism of action. They are actively trying to:

Identify cell-surface receptors: Determine ⁤which receptors BRP binds to.

Dissect action pathways: Elucidate the specific signaling pathways activated‍ by⁣ BRP within cells.

The initial study showed that BRP activates different pathways than GLP-1⁤ and semaglutide.

What is the potential of BRP as an anti-obesity treatment?

BRP’s ability to reduce food intake, promote fat loss, and improve glucose and insulin tolerance in ‍animal models suggests it has significant potential as ‍an anti-obesity treatment. Svensson notes that⁢ existing ⁢treatments haven’t matched semaglutide’s results in appetite and weight reduction, emphasizing the importance of determining ⁣BRP’s safety and effectiveness in humans.

What are the next steps in BRP research?

Future research directions include:

‍ Identifying the specific cell-surface‍ receptors that bind to BRP.

Further dissecting BRP’s⁣ action pathways to understand how it works at ⁢a molecular level.

Exploring methods to prolong the peptide’s effects ‍for a more convenient dosing schedule.

Most ⁣importantly, determining if BRP is safe and effective in humans through clinical trials.

Who is ⁢involved in the BRP research?

The⁢ research is a collaborative effort ⁤involving researchers⁤ from:

⁤ University of California,⁣ Berkeley

University‍ of Minnesota

University⁤ of British Columbia

What funding sources support this research?

The study received funding from⁣ various prominent sources, including:

⁢National Institutes ⁣of Health (NIH)

SPARK Translational Research Program at Stanford

Stanford Bio-X

Stanford Maternal and Child ⁣Health Research Institute

⁣ ‍American Heart Association

Stanford Medicine Dean’s Fellowship Award

Carlsberg Foundation

⁤ Wu Tsai⁣ Human Performance Alliance

Are there any conflicts of interest to be ‍aware of?

Yes, ⁣it’s ⁢important ⁣to⁣ note that Svensson and Coassolo are inventors on patents regarding‍ BRP peptides for‍ metabolic disorders. Svensson is also a co-founder ⁤of ⁤Merrifield‍ Therapeutics. This disclosure ensures⁢ openness regarding potential⁤ biases.

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